Rapid Whole-Exome Sequencing As a Diagnostic Tool in a Neonatal/Pediatric Intensive Care Unit

Overview

Journal J Clin Med

Specialty General Medicine

Date 2020 Jul 17

PMID 32668698

Citations 30

Authors

Robert Smigiel

Mateusz Biela

Krzysztof Szmyd

Michal Bloch

Elzbieta Szmida

Pawel Skiba

Anna Walczak

Piotr Gasperowicz

Joanna Kosinska

Malgorzata Rydzanicz

Piotr Stawinski

Anna Biernacka

Marzena Zielinska

Waldemar Golebiowski

Agnieszka Jalowska

Grazyna Ohia

Bozena Glowska

Wojciech Walas

Barbara Krolak-Olejnik

Pawel Krajewski

Jolanta Sykut-Cegielska

Maria M Sasiadek

Rafal Ploski

Affiliations

Soon will be listed here.

Abstract

Genetic disorders are the leading cause of infant morbidity and mortality. Due to the large number of genetic diseases, molecular and phenotype heterogeneity and often severe course, these diseases remain undiagnosed. In infants with a suspected acute monogenic disease, rapid whole-exome sequencing (R-WES) can be successfully performed. R-WES (singletons) was performed in 18 unrelated infants with a severe and/or progressing disease with the suspicion of genetic origin hospitalized in an Intensive Care Unit (ICU). Blood samples were also collected from the parents. The results from the R-WES were available after 5-14 days. A conclusive genetic diagnosis was obtained in 13 children, corresponding to an overall diagnostic yield of 72.2%. For nine patients, R-WES was used as a first-tier test. Eight patients were diagnosed with inborn errors of metabolism, mainly mitochondrial diseases. In two patients, the disease was possibly caused by variants in genes which so far have not been associated with human disease ( and ). R-WES proved to be an effective diagnostic tool for critically ill infants in ICUs suspected of having a genetic disorder. It also should be considered as a first-tier test after precise clinical description. The quickly obtained diagnosis impacts patient's medical management, and families can receive genetic counseling.

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